Soyyigit Sadan, Guloglu Deniz, Ikinciogullari Aydan, Secil Derya, Oztuna Derya, Mungan Dilsad, Misirligil Zeynep, Sin Betul Ayse
Division of Immunology and Allergic Diseases, Department of Chest Diseases, Ankara University, School of Medicine, Ankara, Turkey.
Department of Pediatric Immunology and Allergy, Ankara University, School of Medicine, Ankara, Turkey.
Ann Allergy Asthma Immunol. 2016 Mar;116(3):244-251.e2. doi: 10.1016/j.anai.2016.01.002.
There is a continuing debate about whether monoallergen subcutaneous immunotherapy (SCIT) is able to modulate immune and clinical responses toward main causal allergen in polysensitized patients.
To investigate short-term immunologic changes and clinical effectiveness of SCIT with Dermatophagoides pteronyssinus in monosensitized and polysensitized patients who have rhinitis with or without asthma.
Nineteen monosensitized and 24 polysensitized patients participated in this prospective, self-placebo-controlled, interventional study. Cluster immunotherapy with D pteronyssinus was administered after 2 months of placebo in both groups. Immunologic parameters, including CD203c expression on basophils after allergen stimulation, total IgE, specific IgE, and specific IgG4, were evaluated at baseline, after placebo, and after immunotherapy. Clinical effectiveness was assessed using monthly symptom-medication scores, visual analog scale, quality-of-life questionnaire, and nasal allergen provocation test.
At baseline, polysensitized patients had higher CD203c expression on basophils than monosensitized patients (P = .007). Activated basophils expressing CD203c, total IgE, and specific IgG4 were significantly increased after immunotherapy compared with baseline and placebo in the polysensitized group (P < .025). After immunotherapy, specific IgE and D pteronyssinus-induced CD203c expression were significantly higher in polysensitized than monosensitized patients (P < .05). The total symptom scores and the Mini Rhinoconjunctivitis Quality of Life Questionnaire scores in polysensitized patients and the visual analog scale scores in both groups were lower after immunotherapy compared with baseline and placebo (P < .025). Titrated nasal allergen provocation test with D pteronyssinus increased after immunotherapy in the monosensitized group (P < .05).
This study indicates that monosensitized and polysensitized patients have distinct humoral response and basophil behavior to SCIT. However, a single-allergen immunotherapy corresponding to the most clinically troublesome allergy in polysensitized patients can lead to early clinical efficacy comparable to that seen in monosensitized patients.
clinicaltrials.gov Identifier: NCT01795846.
关于单过敏原皮下免疫疗法(SCIT)是否能够调节多敏患者对主要致病过敏原的免疫和临床反应,一直存在争议。
研究对患有鼻炎伴或不伴哮喘的单敏和多敏患者,采用尘螨皮下免疫疗法(SCIT)的短期免疫变化和临床疗效。
19名单敏患者和24名多敏患者参与了这项前瞻性、自身安慰剂对照的干预性研究。两组在接受2个月安慰剂治疗后,均给予尘螨集群免疫疗法。在基线、安慰剂治疗后和免疫治疗后,评估免疫参数,包括过敏原刺激后嗜碱性粒细胞上CD203c的表达、总IgE、特异性IgE和特异性IgG4。使用每月症状-用药评分、视觉模拟量表、生活质量问卷和鼻过敏原激发试验评估临床疗效。
在基线时,多敏患者嗜碱性粒细胞上的CD203c表达高于单敏患者(P = 0.007)。与基线和安慰剂相比,多敏组免疫治疗后表达CD203c的活化嗜碱性粒细胞、总IgE和特异性IgG4显著增加(P < 0.025)。免疫治疗后,多敏患者的特异性IgE和尘螨诱导的CD203c表达显著高于单敏患者(P < 0.05)。与基线和安慰剂相比,多敏患者的总症状评分和迷你鼻结膜炎生活质量问卷评分以及两组的视觉模拟量表评分在免疫治疗后均降低(P < 0.025)。单敏组免疫治疗后,尘螨滴定鼻过敏原激发试验增加(P < 0.05)。
本研究表明,单敏和多敏患者对SCIT有不同的体液反应和嗜碱性粒细胞行为。然而,针对多敏患者临床上最麻烦的过敏进行的单一过敏原免疫疗法可导致与单敏患者相当的早期临床疗效。
clinicaltrials.gov标识符:NCT01795846。